A molecular view of liver regeneration

Tarlá, Marissa Rabelo; Ramalho, Fernando Silva; Ramalho, Leandra Naíra Zambelli; Silva, Tiago de Castro e; Brandão, Daniel Ferracioli; Ferreira, Juliana; Silva, Orlando de Castro e; Zucoloto, Sérgio

doi:10.1590/s0102-86502006000700014

Cited by 22 publications

(29 citation statements)

References 28 publications

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“…Since hepatic regeneration in rodents is similar to that observed in humans, the results obtained from rodents can be also applicable to the human liver 18 . The priming stage (G 0 /G 1 transition) comprises the first 4-6 h, followed by progression that lasts 12-16 h. Hepatic DNA synthesis (S phase) starts around 18 h and peaks at 24 h after surgery [12][13][14] . Cell proliferation has been suggested to involve a regulated passage through some checkpoints which ensure the proper timing of cell cycle events 19 .…”

Section: Discussionmentioning

confidence: 99%

“…The first stage (priming), in which hepatocytes undergo transition from resting state (G 0 ) to one in which they become capable to proliferate (G 1 ), lasts 4-6 h after PH 14 . Then, these primed hepatocytes enter a progression stage, with DNA synthesis starting around 18 h and peaking at 24 h after PH [12][13][14] . The objective of the present study was to investigate the effect of FOH administration in rats submitted to PH, a synchronized and well caracterized model for the study of cell proliferation.…”

Section: Introductionmentioning

confidence: 99%

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Farnesol inhibits cell proliferation and induces apoptosis after partial hepatectomy in rats

Chagas¹,

Vieira²,

Ong³

et al. 2009

Acta Cir. Bras.

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Purpose:To study farnesol (FOH) effects on liver regeneration after 70% partial hepatectomy (PH) in rats. Methods: Animals received FOH (25 mg/100 g body weight/day) or corn oil (CO, 0.25 mL/100 g body weight/day, controls). After a 2 week-treatment, all animals were subjected to PH and euthanized at different time points (0 h, 0.5 h, 4 h, 8 h, 18 h and 24 h) after surgery. Hepatic cell proliferation (PCNA positive nuclei) and apoptosis (fluorescence microscopy) were evaluated. Results: Compared to CO treatment, FOH treatment inhibited (p<0.05) cell proliferation at 24h (S phase of the cell cycle) after PH. This was preceded by an induction of apoptosis 0.5 h (p<0.05; G 0 /G 1 transition phase) after surgery. Conclusion: The results of the present study suggest that apoptosis induction could be associated with the reduced number of cells at the S phase observed in FOH group. These novel in vivo data reinforce FOH as a promising chemopreventive and therapeutic agent against cancer. Key words: Farnesol. Hepatectomy. Cell Proliferation. Apoptosis. Rats. RESUMO Objetivo:Estudar o efeito do farnesol (FOH) durante a regeneração hepática em ratos submetidos à Hepatectomia Parcial (HP) a 70%. Métodos: Os animais foram tratados com FOH (25 mg/100g de peso corpórel/dia) ou óleo de milho (OM, 0,25 mL/100g de peso corpóreo/dia, grupo controle). Depois de 2 semanas de tratamento, todos os animais foram submetidos à HP e eutanaziados em diferentes momentos (0h, 30min., 4h, 8h, 18h, 24h.) após o procedimento cirúrgico. Foi avaliada a proliferação celular (imunohistoquímica para PCNA) e a apoptose (microscopia de fluorescência). Resultados: Em comparação aos animais controles, animais tratados com FOH apresentaram menor (p<0,05) proliferação celular 24h. (fase S do ciclo celular) após a HP. Tal efeito foi precedido de uma indução de apoptose 30min. (p<0,05; transição entre as fases G 0 /G 1 do ciclo celular) após a cirurgia. Conclusão: Os resultados do presente estudo sugerem que a indução da apoptose pode estar associada com o menor número de células na fase S observadas nos animais tratados com FOH. Essa nova evidência in vivo reforça o farnesol como um promissor agente preventivo e terapêutico contra o câncer. Descritores: Farnesol. Hepatectomia. Proliferação de Células. Apoptose. Ratos.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Farnesol inhibits cell proliferation and induces apoptosis after partial hepatectomy in rats

Chagas¹,

Vieira²,

Ong³

et al. 2009

Acta Cir. Bras.

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“…ECM compounds can even perform cleavage of the humoral factors to increase or limit their function (54).…”

Section: On the Normal Architecture And Function Of The Livermentioning

confidence: 99%

Studying Liver Regeneration by Means of Molecular Biology: How Far We Are in Interpreting the Findings?

Rychtrmoc

Libra

Bunček

et al. 2009

Acta Med. (Hradec Kralove, Czech Repub.)

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Summary: Liver regeneration in mammals is a unique phenomenon attracting scientific interest for decades. It is a valuable model for basic biology research of cell cycle control as well as for clinically oriented studies of wide and heterogeneous group of liver diseases. This article provides a concise review of current knowledge about the liver regeneration, focusing mainly on rat partial hepatectomy model. The three main recognized phases of the regenerative response are described. The article also summarizes history of molecular biology approaches to the topic and finally comments on obstacles in interpreting the data obtained from large scale microarray-based gene expression analyses.

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“…Basicamente a estrutura do parênquima hepático está organizada em lobos que contém uma veia central, circundada por seis espaços portais (RAO, 2003;TARLÁ et al, 2006a).…”

Section: Histologia E Fisiologia Hepáticaunclassified

“…Oxigenação hiperbárica (OZDOGAN et al, 2005). Transplante hepático; emprego de células tronco hepática (TARLÁ et al, 2006a). Parra et al (1992) testaram uma solução de fatores hepatotróficos em ratas com fígados normais, baseada em uma solução hospitalar de nutrição parenteral, com aminoácidos, vitaminas e sais minerais; administraram-na por via intraperitoneal (portal), foi observado aumento de 34,5% da massa hepática.…”

Section: Introductionunclassified

Avaliação morfológica e molecular pós-tratamento com os fatores hepatotróficos, da cirrose hepática induzida em ratas pela tioacetamida: análise a curto e longo prazo

Silva¹

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A Deus e a minha Mãezinha do Céu, Por terem me concedido o dom da perseverança.Meus queridos pais José Reis da Silva e Iracilda Donizete dos Anjos Silva "Nena", Mesmo distantes, agradeço imensamente ao AMOR compartilhado, os conselhos e ensinamentos das conquistas dos objetivos com muita dignidade.Meus irmãos "Clau e Suzi", Claudio Reis dos Anjos Silva e Suziane dos Anjos Silva pelo apoio participado.Meus sobrinhos Alexander, Ígor e Vítor, Meus três anjos me ensinaram que nas dificuldades o bom mesmo é olhar pra trás e lembrar que um dia eu também fui criança e que com o passar dos anos a gente se torna grande e capaz o suficiente pra poder vencer e enfrentar tudo.Aos meus avós, Germano Moreira dos Anjos (in memorian) e Regina Aparecida Botura dos Anjos, Pelo ensinamento do dom da vida. AGRADECIMENTOS ESPECIAIS

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A molecular view of liver regeneration

Cited by 22 publications

References 28 publications

Farnesol inhibits cell proliferation and induces apoptosis after partial hepatectomy in rats

Farnesol inhibits cell proliferation and induces apoptosis after partial hepatectomy in rats

Studying Liver Regeneration by Means of Molecular Biology: How Far We Are in Interpreting the Findings?

Avaliação morfológica e molecular pós-tratamento com os fatores hepatotróficos, da cirrose hepática induzida em ratas pela tioacetamida: análise a curto e longo prazo

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